Origin of neointimal endothelium and α-actin–positive smooth muscle cells in transplant arteriosclerosis
Jan-Luuk Hillebrands, … , Paul Nieuwenhuis, Jan Rozing
Jan-Luuk Hillebrands, … , Paul Nieuwenhuis, Jan Rozing
Published June 1, 2001
Citation Information: J Clin Invest. 2001;107(11):1411-1422. https://doi.org/10.1172/JCI10233.
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Origin of neointimal endothelium and α-actin–positive smooth muscle cells in transplant arteriosclerosis

Abstract

The development of transplant arteriosclerosis (TA) is today’s most important problem in clinical organ transplantation. Histologically, TA is characterized by perivascular inflammation and progressive intimal thickening. Current thought on this process of vascular remodeling assumes that neointimal vascular smooth muscle (VSM) cells and endothelium in TA are graft-derived, holding that medial VSM cells proliferate and migrate into the subendothelial space in response to signals from inflammatory cells and damaged graft endothelium. Using MHC class I haplotype-specific immunohistochemical staining and single-cell PCR analyses, we show that the neointimal α-actin–positive VSM cells in rat aortic or cardiac allografts are of recipient and not of donor origin. In aortic but not in cardiac allografts, recipient-derived endothelial cells (ECs) replaced donor endothelium. Cyclosporine treatment prevents neointima formation and preserves the vascular media in aortic allografts. Recipient-derived ECs do not replace graft endothelium after cyclosporine treatment. We propose that, although it progresses beyond the needs of functional repair, TA reflects the activity of a normal healing process that restores vascular wall function following allograft-induced immunological injury.

Authors

Jan-Luuk Hillebrands, Flip A. Klatter, Bart M.H. van den Hurk, Eliane R. Popa, Paul Nieuwenhuis, Jan Rozing

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Figure 3

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Neointimal ECs in cardiac allografts are of donor origin. Immunohistoche...
Neointimal ECs in cardiac allografts are of donor origin. Immunohistochemical staining was performed on nontransplanted AO cardiac tissue (ae) and PVG allografts (fj). (a) Medial VSM cells are α-actin–positive in CAs in normal, nontransplanted AO cardiac tissue. (b) ECs are covering the internal elastic lamina as indicated by positive RECA-1 staining. (c) MHC class I expression on ECs was confirmed by positive staining using OX18. (d) U9F4 is AO MHC class I haplotype-specific and recognizes AO-derived ECs. (e) OX27 does not recognize AO-derived ECs. PVG cardiac allografts transplanted in AO recipients showed severe TA 530 days after transplantation. The vascular lumen is obliterated as a result of neointima formation. (f) Neointimal tissue predominantly consists of α-actin–positive VSM cells. (g) Neointima is covered by RECA-1–positive ECs. Note the swollen and activated appearance of the neointimal ECs. (h) MHC class I expression on ECs was confirmed by positive staining using OX18. (i) Neointimal ECs are U9F4-negative, indicating donor origin. (j) Positive OX27 staining confirmed donor origin of neointimal ECs in CAs with severe TA. Arrowheads indicate positively stained ECs. m, media; ni, neointima. Original magnification: ×400.